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被同种异体反应性T淋巴细胞克隆识别的自身主要组织相容性复合体(Self-MHC)限制肽。

Self-MHC-restricted peptides recognized by an alloreactive T lymphocyte clone.

作者信息

Udaka K, Wiesmüller K H, Kienle S, Jung G, Walden P

机构信息

Max Planck Institute for Biology, Immunogenetics Section, Tübingen, Germany.

出版信息

J Immunol. 1996 Jul 15;157(2):670-8.

PMID:8752916
Abstract

Alloreactive T lymphocytes are readily detected in unprimed animals although they have never encountered the alloantigen before. This well-established phenomenon is usually explained with the assumption that a self-MHC molecule complexed with a defined peptide resembles the allo-MHC molecule with another peptide and induces the corresponding T cell specificities. Here, for the first time and in support of this hypothesis, self-MHC-restricted peptides are described for a T cell clone that was induced with allo-MHC. The allo-MHC-specific CTL clone 2C was derived from a H-2b mouse and recognizes H-2Ld complexed with the naturally occurring endogenous peptide LSPFPFDL. H-2Kb was shown to be involved in positive selection of its TCR, and peptides associated with this MHC molecule are implicated in the process. To identify such peptides, positional scanning with random peptide libraries combined with an iterative approach was employed. Several active peptides were found and the most efficient, SIYRYYGL, was chosen for further studies. Recognition by 2C of the two MHC-peptide adducts H-2Ld + LSPFPFDL and H-2Kb + SIYRYYGL is mediated by the same TCR and appears to be similarly efficient as concluded from inhibition experiments with an Id-specific Ab. CTLs from SIYRYYGL-primed H-2b mice respond to H-2Ld + LSPFPFDL. This reciprocal cross-reactivity suggests that structural features are shared by the two MHC-peptide complexes.

摘要

在未经致敏的动物中很容易检测到同种反应性T淋巴细胞,尽管它们以前从未接触过同种抗原。这种已被充分证实的现象通常用这样的假设来解释,即与特定肽结合的自身MHC分子类似于与另一种肽结合的同种MHC分子,并诱导相应的T细胞特异性。在此,首次描述了一种由同种MHC诱导的T细胞克隆的自身MHC限制性肽,以支持这一假设。同种MHC特异性CTL克隆2C源自H-2b小鼠,可识别与天然存在的内源性肽LSPFPFDL结合的H-2Ld。已证明H-2Kb参与其TCR的阳性选择,并且与该MHC分子相关的肽也参与了这一过程。为了鉴定此类肽,采用了随机肽库的位置扫描结合迭代方法。发现了几种活性肽,并选择了最有效的SIYRYYGL进行进一步研究。2C对两种MHC-肽加合物H-2Ld + LSPFPFDL和H-2Kb + SIYRYYGL的识别由相同的TCR介导,并且从用Id特异性抗体进行抑制实验得出的结论来看,其效率似乎相似。来自用SIYRYYGL致敏的H-2b小鼠的CTL对H-2Ld + LSPFPFDL有反应。这种相互交叉反应表明这两种MHC-肽复合物具有共同的结构特征。

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